Pregabalin administration in patients with fibromyalgia: a Bayesian network meta-analysis

Several studies investigated the effectiveness and the safety of different doses of pregabalin in fibromyalgia. However, the optimal protocol remains controversial. A Bayesian network meta-analysis comparing 300, 450, and 600 mg/daily of pregabalin for fibromyalgia was conducted. The literature search was conducted in January 2022. All the double-blind randomised clinical trials comparing two or more dose protocols of pregabalin for fibromyalgia were accessed. Studies enrolling less than 50 patients were not eligible, nor were those with a length of follow-up shorter than eight weeks. The outcomes of interests were: Fibromyalgia Impact Questionnaire (FIQ), sleep quality, and adverse events. The network meta-analyses were performed using the routine for Bayesian hierarchical random-effects model analysis, with log odd ratio (LOR) and standardized mean difference (SMD) effect measure. Data from 4693 patients (mean age 48.5 years) were retrieved. 93.1% (4370 of 4693 patients) were women. The median follow-up was 14.8 weeks. Pregabalin 450 mg/daily resulted in greater reduction in Fibromyalgia Impact Questionnaire (SMD − 1.83). Pregabalin 600 demonstrated the greatest sleep quality (SMD 0.15). Pregabalin 300 mg/daily evidenced the lowest rate of adverse events (LOR 0.12). The dose of pregabalin must be customised according to patients’ characteristics and main symptoms.


Methods
Search strategy. This Bayesian network meta-analysis was conducted according to the PRISMA extension statement for reporting of systematic reviews incorporating network meta-analyses of health care interventions 23 . The PICOTD framework was preliminary pointed out: • Data source and extraction. The 24 , were considered. Only studies that clearly stated the doses of pregabalin were considered for inclusion. Compounds other than pregabalin were considered as control group. To ensure the reliability of the data to be collected, studies enrolling less than 50 patients were excluded, as were those with a length of follow-up shorter than eight weeks. Reviews, letters, expert opinion, editorials were not considered. Studies combining pregabalin with other compounds were not considered. Missing quantitative data under the outcomes of interest warranted the exclusion from the present study.
Outcomes of interest. Data extraction was performed by two authors (F.M. and G.C.). Study generalities (author, year, and journal) and patient baseline demographic information were extracted (number of samples, mean age, and sex). The following data were extracted: Fibromyalgia Impact Questionnaire (FIQ) total score, mean sleep quality, and adverse events. The mean sleep quality is a numeric rating scale, in which 0 represent the best and 10 the worst possible sleep. The outcomes of interests were to compare 300; 450; 600 mg/daily of pregabalin at last follow-up.
Methodology quality assessment. The methodological quality assessment was performed by two authors (F.M. and G.C.) using the bias graph tool of the Review Manager Software (The Nordic Cochrane Collaboration, Copenhagen). The following risk of bias were evaluated: selection, detection, performance, reporting, attrition and other source of bias.
Statistical analysis. The statistical analysis was performed by the main author (F.M.). The Shapiro-Wilk test was performed to investigate data distribution for baseline assessment. Parametric data were assessed using mean and standard deviation. Non-parametric data were assessed using median and interquartile range. The analysis of variance (ANOVA) and the Kruskal-Wallis test were respectively performed, with values of P > 0.1 considered satisfactory. The network meta-analyses were performed through the STATA Software/MP Version 16 (StataCorporation, College Station, Texas, USA) using the routine for Bayesian hierarchical random-effects model analysis. The inverse variance method was used for all the comparisons. The Log odd ratio (LOR) effect measures was used for dichotomous variables, while the standardized mean difference (SMD) for the continuous variables. The overall inconsistency was evaluated through the equation for global linearity via the Wald test. If P value > 0.1, the null hypothesis could not be rejected, and the consistency assumption is accepted at the overall level of each treatment. Both confidence (CI) and percentile (PrI) intervals were set at 95%. Edge plots, interval plots, funnel plots and ranking plots were obtained and evaluated.
Ethical approval. This study complies with ethical standards.  www.nature.com/scientificreports/ Methodological quality assessment. The random sequence generation and allocation concealment were adequately described and unbiased, leading to a low risk of selection bias. Given the double-blinded nature of the study design of the included studies, the risk of performance and detection were low. The risk of attrition bias of incomplete outcome data was low, as was the risk of reporting bias. The reviewers found no other risk of bias which may exert an influence in the validity of the present study. Concluding, the risk of publication bias was very low, attesting to the present study an optimal methodological quality assessment (Fig. 2).

Results
Patient demographics. Data of 4693 patients were retrieved. 93.1% (4370 of 4693 patients) were women.
The mean age of the patients was 48.5 ± 0.9 years. Only two studies 16,18 reported data concerning the mean BMI, which was 30.0 ± 0.8 kg/m 2 . The median follow-up was 14.8 ± 5.9 weeks. The ANOVA test found good baseline comparability in terms of age, BMI, and gender (P > 0.1). Generalities and demographic of the study are shown in Table 1.  Fig. 3.

Discussion
According to the present Bayesian network meta-analysis, daily administration of 450 mg of pregabalin resulted in the greatest FIQ, while 600 mg/daily was the most effective dose improve sleep quality in fibromyalgia. Patient treated with pregabalin 300 mg/daily experienced the lowest rate of adverse events. The sleep quality was directly proportional to dose escalation. Given the high prevalence and impact, sleep disorders are a key component of fibromyalgia, and patients evidence delayed sleep onset, more frequent arousals and decreased sleep efficiency compared with healthy controls 25 . Polysomnography demonstrated an alpha delta sleep pattern during non-REM phases 26,27 . Administration of 150 to 450 mg/daily of pregabalin for a month improved total sleep time and quality, latency to persistent sleep, the number of awakenings after sleep onset, and the amount of slow-wave sleep relative to placebo 28 . Previous placebo-controlled trials of pregabalin for the treatment of fibromyalgia showed that pregabalin improved daily sleep quality diary (DSQD) and Medical Outcomes Study-Sleep Scale (MOS-SS) scores at doses of 300, 450 and 600 mg/d 17,18,20,21,29,30 . This improvement was evident from the second week, and was sustained throughout the administration period. High association between pain relief and improvement in sleep quality was demonstrated for all doses of pregabalin 17,18,30 . As expected, the rate of adverse event was inversely proportional to the dose escalation. The interval plots reported minimal  www.nature.com/scientificreports/ difference in the effect. Most of CI are overlapping, and the analyses of the FIQ and adverse events revealed wide CI. Moreover, the funnel plots, especially in the analysis of FIQ and sleep quality were well proportioned with a symmetrical distribution of the referral points, which indicates low data dispersion and reliable results. The funnel plot of the adverse events demonstrated greater heterogeneous distribution; however, this endpoint included a wide range of possible complications, from both pharmacological management and natural disease progression. The most commonly reported adverse events included dizziness, headache, and fatigue nausea, blurred vision, and dry mouth and sleep disorders. The management of fibromyalgia is complex 31 . The available guidelines recommend a combined approach of pharmacological and non-pharmacological therapy 32 . Among the pharmacological therapies, pregabalin, duloxetine, and milnacipran have been approved by FDA for fibromyalgia 33 . Clair et al. 14 collected data from five double-blind RCTs concerning the use of pregabalin for fibromyalgia. They evidenced the superiority of pregabalin in improving pain and sleep scores compared to placebo 14 . In the double-blind placebo-controlled RCT conducted by Arnold et al. 17 , 750 patients were allocated to receive pregabalin 300, 450, or 600 mg/daily or placebo. They found that the rate of 30% pain relief was 42% (76 of 183 patients), 50% (94 of 190 patients), and 48% (88 of 188 patients), respectively 17 . The rate of 50% responders was 24% (44 of 183 patients), 27% (52 of 190 patients), and 30% (57 of 188 patients), respectively 17 . Moreover, similarly to the results of the present study, they found greater FIQ improvement with 450 and 600 mg/daily compared to 300 mg/daily 17 . We were not able to identify a previous Bayesian network meta-analysis which compared the administration of different doses of pregabalin for fibromyalgia. The findings of previous head to head meta-analysis were similar to those inferred by the present study. Choy et al. 34 in a meta-analysis found greater FIQ and sleep quality with 450 and 600 mg/daily compared to 300 mg/daily. Similarly, the current study evidenced better sleep quality in patients who take 600 and 450 mg/daily of pregabalin compared to 300 mg/daily. Moore et al. 35 reported no difference between the efficacy of 450 and 600 mg/daily in 30% and 50% pain relief. Likewise, the intake of 300, 450, and 600 mg of pregabalin has similar potential in pain reduction 36 . Also, 150 mg/daily pregabalin promoted similar efficacy and tolerability to placebo 36 . A Bayesian network meta-analysis, not focusing exclusively on pregabalin, found that 300 mg of pregabalin was superior to 150 mg in pain relief 37 . A meta-analysis on 21 RCTs investigated several pharmacological compounds, and compared them to placebo 38 . The number of patients who achieved 30% and 50% pain relief was greater for pregabalin 450 mg/daily than 300 mg/daily. Straube et al. 29 performed a meta-analysis on five RCTs (3808 patients) concerning the administration of pregabalin 150, 300, 450, and  www.nature.com/scientificreports/ 600 mg/daily. 300 to 600 mg/daily produced pain relief in 30% to 50%, while 150 mg/daily demonstrated limited efficacy in 50% pain relief 29 . Similar to the results of the current study, 450 mg/daily of pregabalin demonstrated a greater impact on FIQ total score than 600 mg; the latter resulted more effective to improve sleep quality 29 . The long-term safety and tolerability of pregabalin have been demonstrated in previous studies 39 . Somnolence, dizziness, dry mouth and peripheral oedema are the most frequent adverse events occurring in patients receiving pregabalin 40 . The meta-analysis by Haeuser et al. 36 reported the adverse effects of different doses of pregabalin. The rate of study discontinuation from adverse events was greater for pregabalin 450 and 600 mg/ daily than 300 mg/daily. In a double-blind, placebo-controlled RCT (747 patients) 20 , the occurrence of adverse events was dose-related. These findings agree with those of the present study: the administration of 300 mg/daily of pregabalin resulted in a lower rate of adverse events.
This study has several limitations. Although the current literature includes several studies investigating the potential of pregabalin in fibromyalgia, according to the inclusion criteria, we were able to identify only six RCTs that directly compared different dose regimes. Despite the high quality of the included studies, the relatively small number of patients available for analysis represent an important limitation. Studies with a follow-up shorter than eight weeks were not included for analysis. Moreover, the impact of the follow-up duration on the treatment response was also not investigated. Short follow-up may not be reliable to evaluate the effectiveness and safety of pharmacological management. Fibromyalgia is a chronic condition, and its management requires long term polytherapy. The investigation of the effect of pharmacological therapies should last longer, following the course of the conditon. The current evidence would benefit of longer observational studies. Given the lack and homogeneity of available data in the current literature, it was not possible to evaluate the full impact of pregabalin therapy on pain relief. There were not enough data on pregabalin 150 mg/daily administration to allow further considerations. However, prior studies stated that the efficacy of pregabalin 150 mg/daily was comparable to placebo administration 29,36,37 . Even though several PROMs have been proposed to investigate the therapy efficacy in fibromyalgia 12,41-44 , given the lack of data of the included studies, no further score was reliably available. Considering these limitations, the results of the present study should be considered cautiously. Future studies including larger populations should investigate long term administration of pregabalin in patients with fibromyalgia.

Conclusion
A daily dose of 450 mg of pregabalin resulted most effective in improving FIQ total score, while 600 mg/daily resulted in greater sleep quality. The rate of adverse events was lower for 300 mg/daily than for greater doses. The dose of pregabalin must be customised according to the patient's characteristics. It is likely that the response to pregabalin is genetically determined. To our knowledge, no such studies have been performed, and, together with better understanding of the underlying condition, they should form the basis of future studies to show better personalisation of drug therapy in fibromyalgia patients.

Data availability
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